Literature DB >> 15916762

Cortical neurogenesis enhanced by chronic perinatal hypoxia.

Devon M Fagel1, Yosif Ganat, John Silbereis, Timothy Ebbitt, William Stewart, Heping Zhang, Laura R Ment, Flora M Vaccarino.   

Abstract

Most regions of the mature mammalian brain, including the cerebral cortex, appear to be unable to support the genesis of new neurons. Here, we report that a low level of neurogenesis occurs in the cerebral cortex of the infant mouse brain and is enhanced by chronic perinatal hypoxia. When mice were reared in a low-oxygen environment from postnatal days 3 to 11, approximately 30% of the cortical neurons were lost after the insult; yet this damage was transient. The loss of cortical neuron number, cortical volume, and brain weight were all reversed during the recovery period. At P18, 7 days after the cessation of hypoxia, there was a marked increase in astroglial cell proliferation within the SVZ, as assessed by 5-bromodeoxyuridine (BrdU) incorporation in S-phase cells. One month after BrdU incorporation, 40% more BrdU-positive cells were found in the cerebral cortex of hypoxic-reared as compared to normoxic control mice. Among these newly generated cortical cells, approximately 45% were oligodendrocytes, 35% were astrocytes, and 10% were neurons in both hypoxic and normoxic mice. However, twice as many BrdU-labeled cells expressed neuronal markers in the neocortex in mice recovering from hypoxia as compared to controls. In both hypoxic-reared and normoxic infant/juvenile mice, putative neuroblasts could be seen detaching from the forebrain subventricular zone, migrating through the subcortical white matter and entering the lower cortical layers, 5 to 11 days after their last mitotic division. We suggest that cortical neurogenesis may play a significant role in repairing neuronal losses after neonatal injury.

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Year:  2006        PMID: 15916762     DOI: 10.1016/j.expneurol.2005.04.006

Source DB:  PubMed          Journal:  Exp Neurol        ISSN: 0014-4886            Impact factor:   5.330


  67 in total

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6.  Fgfr1 is required for cortical regeneration and repair after perinatal hypoxia.

Authors:  Devon M Fagel; Yosif Ganat; Elise Cheng; John Silbereis; Yasushi Ohkubo; Laura R Ment; Flora M Vaccarino
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10.  Long-term survival of human neural stem cells in the ischemic rat brain upon transient immunosuppression.

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